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2
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本文引用的文献

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A method to configure protein side-chains from the main-chain trace in homology modelling.一种在同源建模中根据主链轨迹配置蛋白质侧链的方法。
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Estimation of the maximum change in stability of globular proteins upon mutation of a hydrophobic residue to another of smaller size.疏水残基突变为另一个更小尺寸的残基时,球状蛋白质稳定性最大变化的估计。
Protein Sci. 1993 May;2(5):733-8. doi: 10.1002/pro.5560020505.
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Similar hydrophobic replacements of Leu99 and Phe153 within the core of T4 lysozyme have different structural and thermodynamic consequences.T4溶菌酶核心区域内Leu99和Phe153类似的疏水取代具有不同的结构和热力学结果。
J Mol Biol. 1993 Feb 5;229(3):747-69. doi: 10.1006/jmbi.1993.1077.
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Shape complementarity at protein/protein interfaces.蛋白质/蛋白质界面处的形状互补性。
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Structural mechanisms for domain movements in proteins.蛋白质中结构域运动的结构机制。
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Anatomy and dynamics of a ligand-binding pathway in myoglobin: the roles of residues 45, 60, 64, and 68.肌红蛋白中配体结合途径的解剖结构与动力学:45、60、64和68位残基的作用
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Intramolecular cavities in globular proteins.球状蛋白质中的分子内空腔。
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A role for surface hydrophobicity in protein-protein recognition.表面疏水性在蛋白质-蛋白质识别中的作用。
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An analysis of packing in the protein folding problem.蛋白质折叠问题中的堆积分析。
Q Rev Biophys. 1993 Nov;26(4):423-98. doi: 10.1017/s0033583500002845.
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Shape complementarity at protein-protein interfaces.蛋白质-蛋白质界面处的形状互补性。
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蛋白质界面处的空洞与堆积

Cavities and packing at protein interfaces.

作者信息

Hubbard S J, Argos P

机构信息

European Molecular Biology Laboratory, Heidelberg, Germany.

出版信息

Protein Sci. 1994 Dec;3(12):2194-206. doi: 10.1002/pro.5560031205.

DOI:10.1002/pro.5560031205
PMID:7756979
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2142764/
Abstract

An analysis of internal packing defects or "cavities" (both empty and water-containing) within protein structures has been undertaken and includes 3 cavity classes: within domains, between domains, and between protein subunits. We confirm several basic features common to all cavity types but also find a number of new characteristics, including those that distinguish the classes. The total cavity volume remains only a small fraction of the total protein volume and yet increases with protein size. Water-filled "cavities" possess a more polar surface and are typically larger. Their constituent waters are necessary to satisfy the local hydrogen bonding potential. Cavity-surrounding atoms are observed to be, on average, less flexible than their environments. Intersubunit and interdomain cavities are on average larger than the intradomain cavities, occupy a larger fraction of their resident surfaces, and are more frequently water-filled. We observe increased cavity volume at domain-domain interfaces involved with shear type domain motions. The significance of interfacial cavities upon subunit and domain shape complementarity and the protein docking problem, as well as in their structural and functional role in oligomeric proteins, will be discussed. The results concerning cavity size, polarity, solvation, general abundance, and residue type constituency should provide useful guidelines for protein modeling and design.

摘要

我们对蛋白质结构内部的堆积缺陷或“空洞”(包括空的和含水的)进行了分析,共包括3类空洞:结构域内、结构域之间以及蛋白质亚基之间。我们确认了所有空洞类型共有的几个基本特征,但也发现了许多新特性,包括区分这些类别的特性。空洞总体积仅占蛋白质总体积的一小部分,但会随着蛋白质大小的增加而增大。充满水的“空洞”具有更具极性的表面,通常也更大。其所含的水对于满足局部氢键潜力是必要的。观察发现,围绕空洞的原子平均而言比其周围环境的柔韧性更低。亚基间和结构域间的空洞平均比结构域内的空洞更大,在其所在表面中占比更大,并且更常充满水。我们观察到,在涉及剪切型结构域运动的结构域-结构域界面处,空洞体积增加。将讨论界面空洞在亚基和结构域形状互补性及蛋白质对接问题中的重要性,以及它们在寡聚蛋白中的结构和功能作用。有关空洞大小、极性、溶剂化、总体丰度和残基类型组成的结果应为蛋白质建模和设计提供有用的指导。